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Regulation of Cell
Cycle
By – Mohit Kumar
overview
• Described by Howard and Pelc in 1953.
• From single cell, zygote to adult cell requires a
series of cell division known as ‘cell cycle’.
Division cycles
• Somatic division cycle: used to fulfill specific requirements.
• Embryonic cycle: having lack of G1 and G2 phase.
• Meiotic cell cycle: allow formation of haploid gametes.
• Endoreduplication: S phase is not followed by mitosis.
Human cell cycle
• Length of cell cycle is highly variable, even within cells of a
single organism.
• In human, frequency of cell turnover range few hours in early
embryonic development to an average of two to five days for
epithelial cells.
• In human, rapidly cell cycle length is about 24 hours.
 G1 phase lasts approximately nine hours.
 S phase lasts ten hours.
 G2 phase lasts about four and one-half hours.
 M phase lasts approximately one-half hour.
Factors that affects cell cycle regulation
• The death of nearby cells.
• As sweeping as the release of growth promoting hormones.
• Crowding of cells.
• Size of the cell during division (decreasing surface to volume
ratio).
• Chromosomal mutation
Checkpoints
• A checkpoint is one of several points in the eukaryotic cell
cycle at which the development of a cell to the next stage in
the cycle can be halted until conditions are favorable.
• These checkpoints occur near the end of G1, at the G2/M
transition, and during the metaphase.
G1 checkpoint
• Also known as restriction point in yeast.
• Check for genomic DNA damage.
• Plays crucial role at this check post due to proliferation of the
cell.
• The cell can halt the cycle and waits, whether to moves G°
phase or signal to improves condition.
G2 checkpoint
• Entry into mitotic phase.
• Whether chromosome have been replicated properly.
• No DNA damage occurs, if occurs than repair
mechanism repair the mutation and completes proper
replication.
M checkpoint
• Known as spindle checkpoint.
• At the end of metaphase in interphase.
• Sister chromatids are correctly attached to the
microtubule or not.
• Cycle get arrested if spindle fiber attached chromatids
doesn’t moves at poles.
cyclins and cyclin-dependent kinases (CDKs)
CDKs
• Master regulator of cell cycle.
• Role is to phosphorylate protien on ‘Ser’ and ‘Thr’ amino
acids.
• Yeast having 1 CDK while animals having 9 CDKs.
Cyclins
• Regulatory subunits of complexes with kinase activity (with
Cdks).
• Their presence “oscillates” in the cell cycle.
• There are G-1cyclin, G1-S cyclin, S cyclin and M cyclin.
Cyclins and CDKs in vertebrates
Activation of CDKs-cyclin complex
Regulation of activity of cyclin-CDKs complex's
• Cyclins undergo a cycle of synthesis and degradation
in each cell cycle, while CDKs level remains constant
during the cell cycle.
• Cyclins-CDKs complex inactivated by regulated
proteolysis of cyclin at specific cell cycle stage.
• Cyclin level in cells are controlled not only by
changes in cyclin destructions but also by changes in
cyclin synthesis.
M-CDKs
• They are mitosis promoting factor or maturation
promoting factor (MPF).
• Synthesized during S and G-2 phase
• Include chromosomal condensation.
• Breakdown of nuclear envelop
• Assembly of mitotic spindle apparatus.
• Alignment of condensed chromosome at metaphase
plate.
• It phosphorylate number of protein such as
condensin, lamin etc.
Regulation of CDKs-cyclin in S. pombe
• After the proper association of chromosomes
with spindle microtubules, the M-CDKs
complexes activates the anaphase promoting
complex/cyclosome (APC/C).
• APC/C acts on different substrate at different
time. It bears to different co activators i.e.
cdc20 and cdh1.
Inactivation of cyclin-CDKs complex's
Inactivation of CDKs –cyclin complex
• Occurs by ubiquitin dependent proteolysis.
• Proteolysis of cyclin is catalyzed by ubiquitin lygase.
• Enzyme SCF(SKp1, cullin, F-box) & E3 ubiquitin
lygase responsible for destruction of G1 phase cyclin.
• E-3 ubiquitin ligase- anaphase promoting
complex/cyclosome (APC/C) is responsible for S&M
phase cyclin inactivation.
Role of Rb protein in cell cycle regulation
• RB1(retinoblastoma) gene encodes Rb protein
of 110 KDa.
• It is a tumor suppressor protein and loss of
function mutation in Rb1 gene leads tumor.
• It is present on 13q14.2 chromosome location.
Rb protein
• Its active, un or hypophosporylated form
binds with E2-F transcription factor and
suppress the gene transcription which is
required for transition from G1 to S phase.
• The product of these genes are required for S
phase of the cell cycle.
• Cyclin-D – CDKs 4/6 phosphorylate the Rb
protein results losses its affinity with EF-2.
Rb protein
• Restriction point: This site ensure that the transition
is responsive to extracellular signals.
• Then cyclin E level is increase, cyclin-E +CDK-2
complex drives fully Phosphorylated form of Rb
protein due to that E2F is released.
• E2F binds with DP(DNA binding protein) &
transcription translation could occurs.
p53 protein
• Tp53 gene encodes for p53 protein of molecular mass
of 53KDa.
• It is also a tumor suppressor gene encodes a
polypeptide chain of 393 amino acid residue.
• It is described as Guardian of the genome &
cellular gatekeeper because it involves in the
complex network of cellular events
• It regulates the expression of several genes involves
in DNA repair, apoptosis, cell growth, antioxidant
defense etc.
p53 protein
• p53 is inactivated by its –ve regulator MDM2 (mouse
double minute 2).
• MDM2 functions as E3 ubiquitin ligase & cause
proteosomal degradation of p53 protein.
• Upon DNA damage or other stress leads to
dissociation of p53 and MDM2 complex, activated
p53 will induce a cell cycle arrest to either repair and
survival of the cell or apoptosis.
pP53 protein
• In double stranded DNA break, protein kinase ATM is
activated which in turn activates CHK 2 kinase.
• Both ATM &CHK2 phosphorylate p53 at distinct sites. At the
same time ATM phosphorylate MDM2 in way that cause its
functional inactivation.
• Phosphorylated p53 acts as transcription factor for p21 gene.
• p21 protein binds with G1/S-CDK and S CDK complexes and
inhibit their activity, thereby helping to block entry into the
cell cycle.
• Hence, p53 level is increase and arrest the cell in the G1 phase
of the cell cycle.
Ubiquitin mediated protein degradation
• Mainly two type of proteolytic system are there:
1. Lysosome mediated- membrane bound + acid
hydrolysis including many proteolytic enzyme.
2. Proteasome mediated- regulated breakdown of
protein by energy dependent manner.
Proteasome
• Found in both prokaryotes and eukaryotes.
• In eukaryotes they present in both cytosol and
nucleus.
• In eukaryotes they are of two types:
 20S Proteasome- cylindrical barrel shaped structure
arranged as four rings in heptamer form upon one
another.
 26S Proteasome- it catalysis the ATP-dependent
degradation of polyubiquitinated proteins.
Ubiquitination
• Most well established means of targeting protein to
proteasome is by addition of ubiquitin.
• Ubiquitin is highly conserved protein of 76 amino acid residue
and covalently attached to a lysine residue on a target protein.
• Protein can be monoubiquitinated, multiubiquitinated or
polyubiquitinated.
Activation of ubiquitin
• Activated by ubiquitin E-1 (ubiquitin activating
enzyme), in energy dependent manner E-1 attach to
ubiquitin at C- terminal.
• Then, E-1 transfer to a ‘cysteine residue’ present on
an E-2 (ubiquitin conjugating enzyme).
• Finally E-3 (ubiquitin ligase)transferred the activated
ubiquitin from E-2 to a lysine amino acid residue of
its target protein, forming an isopeptide bond.
Attractions:
• Cell cycle
• Checkpoints
• Activation/inactivation of cyclin-cdks complex
• Rb protein
• P53 protein
• Ubiquitin mediated proteasomal degradation

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Regulation of cell cycle

  • 1. Regulation of Cell Cycle By – Mohit Kumar
  • 2. overview • Described by Howard and Pelc in 1953. • From single cell, zygote to adult cell requires a series of cell division known as ‘cell cycle’.
  • 3. Division cycles • Somatic division cycle: used to fulfill specific requirements. • Embryonic cycle: having lack of G1 and G2 phase. • Meiotic cell cycle: allow formation of haploid gametes. • Endoreduplication: S phase is not followed by mitosis.
  • 4. Human cell cycle • Length of cell cycle is highly variable, even within cells of a single organism. • In human, frequency of cell turnover range few hours in early embryonic development to an average of two to five days for epithelial cells. • In human, rapidly cell cycle length is about 24 hours.  G1 phase lasts approximately nine hours.  S phase lasts ten hours.  G2 phase lasts about four and one-half hours.  M phase lasts approximately one-half hour.
  • 5. Factors that affects cell cycle regulation • The death of nearby cells. • As sweeping as the release of growth promoting hormones. • Crowding of cells. • Size of the cell during division (decreasing surface to volume ratio). • Chromosomal mutation
  • 6. Checkpoints • A checkpoint is one of several points in the eukaryotic cell cycle at which the development of a cell to the next stage in the cycle can be halted until conditions are favorable. • These checkpoints occur near the end of G1, at the G2/M transition, and during the metaphase.
  • 7. G1 checkpoint • Also known as restriction point in yeast. • Check for genomic DNA damage. • Plays crucial role at this check post due to proliferation of the cell. • The cell can halt the cycle and waits, whether to moves G° phase or signal to improves condition.
  • 8. G2 checkpoint • Entry into mitotic phase. • Whether chromosome have been replicated properly. • No DNA damage occurs, if occurs than repair mechanism repair the mutation and completes proper replication.
  • 9. M checkpoint • Known as spindle checkpoint. • At the end of metaphase in interphase. • Sister chromatids are correctly attached to the microtubule or not. • Cycle get arrested if spindle fiber attached chromatids doesn’t moves at poles.
  • 10. cyclins and cyclin-dependent kinases (CDKs) CDKs • Master regulator of cell cycle. • Role is to phosphorylate protien on ‘Ser’ and ‘Thr’ amino acids. • Yeast having 1 CDK while animals having 9 CDKs. Cyclins • Regulatory subunits of complexes with kinase activity (with Cdks). • Their presence “oscillates” in the cell cycle. • There are G-1cyclin, G1-S cyclin, S cyclin and M cyclin.
  • 11.
  • 12. Cyclins and CDKs in vertebrates
  • 13.
  • 15. Regulation of activity of cyclin-CDKs complex's • Cyclins undergo a cycle of synthesis and degradation in each cell cycle, while CDKs level remains constant during the cell cycle. • Cyclins-CDKs complex inactivated by regulated proteolysis of cyclin at specific cell cycle stage. • Cyclin level in cells are controlled not only by changes in cyclin destructions but also by changes in cyclin synthesis.
  • 16. M-CDKs • They are mitosis promoting factor or maturation promoting factor (MPF). • Synthesized during S and G-2 phase • Include chromosomal condensation. • Breakdown of nuclear envelop • Assembly of mitotic spindle apparatus. • Alignment of condensed chromosome at metaphase plate. • It phosphorylate number of protein such as condensin, lamin etc.
  • 18. • After the proper association of chromosomes with spindle microtubules, the M-CDKs complexes activates the anaphase promoting complex/cyclosome (APC/C). • APC/C acts on different substrate at different time. It bears to different co activators i.e. cdc20 and cdh1.
  • 19.
  • 21. Inactivation of CDKs –cyclin complex • Occurs by ubiquitin dependent proteolysis. • Proteolysis of cyclin is catalyzed by ubiquitin lygase. • Enzyme SCF(SKp1, cullin, F-box) & E3 ubiquitin lygase responsible for destruction of G1 phase cyclin. • E-3 ubiquitin ligase- anaphase promoting complex/cyclosome (APC/C) is responsible for S&M phase cyclin inactivation.
  • 22. Role of Rb protein in cell cycle regulation • RB1(retinoblastoma) gene encodes Rb protein of 110 KDa. • It is a tumor suppressor protein and loss of function mutation in Rb1 gene leads tumor. • It is present on 13q14.2 chromosome location.
  • 23.
  • 24. Rb protein • Its active, un or hypophosporylated form binds with E2-F transcription factor and suppress the gene transcription which is required for transition from G1 to S phase. • The product of these genes are required for S phase of the cell cycle. • Cyclin-D – CDKs 4/6 phosphorylate the Rb protein results losses its affinity with EF-2.
  • 25. Rb protein • Restriction point: This site ensure that the transition is responsive to extracellular signals. • Then cyclin E level is increase, cyclin-E +CDK-2 complex drives fully Phosphorylated form of Rb protein due to that E2F is released. • E2F binds with DP(DNA binding protein) & transcription translation could occurs.
  • 26. p53 protein • Tp53 gene encodes for p53 protein of molecular mass of 53KDa. • It is also a tumor suppressor gene encodes a polypeptide chain of 393 amino acid residue. • It is described as Guardian of the genome & cellular gatekeeper because it involves in the complex network of cellular events • It regulates the expression of several genes involves in DNA repair, apoptosis, cell growth, antioxidant defense etc.
  • 27. p53 protein • p53 is inactivated by its –ve regulator MDM2 (mouse double minute 2). • MDM2 functions as E3 ubiquitin ligase & cause proteosomal degradation of p53 protein. • Upon DNA damage or other stress leads to dissociation of p53 and MDM2 complex, activated p53 will induce a cell cycle arrest to either repair and survival of the cell or apoptosis.
  • 28.
  • 29.
  • 30. pP53 protein • In double stranded DNA break, protein kinase ATM is activated which in turn activates CHK 2 kinase. • Both ATM &CHK2 phosphorylate p53 at distinct sites. At the same time ATM phosphorylate MDM2 in way that cause its functional inactivation. • Phosphorylated p53 acts as transcription factor for p21 gene. • p21 protein binds with G1/S-CDK and S CDK complexes and inhibit their activity, thereby helping to block entry into the cell cycle. • Hence, p53 level is increase and arrest the cell in the G1 phase of the cell cycle.
  • 31. Ubiquitin mediated protein degradation • Mainly two type of proteolytic system are there: 1. Lysosome mediated- membrane bound + acid hydrolysis including many proteolytic enzyme. 2. Proteasome mediated- regulated breakdown of protein by energy dependent manner.
  • 32. Proteasome • Found in both prokaryotes and eukaryotes. • In eukaryotes they present in both cytosol and nucleus. • In eukaryotes they are of two types:  20S Proteasome- cylindrical barrel shaped structure arranged as four rings in heptamer form upon one another.  26S Proteasome- it catalysis the ATP-dependent degradation of polyubiquitinated proteins.
  • 33.
  • 34. Ubiquitination • Most well established means of targeting protein to proteasome is by addition of ubiquitin. • Ubiquitin is highly conserved protein of 76 amino acid residue and covalently attached to a lysine residue on a target protein. • Protein can be monoubiquitinated, multiubiquitinated or polyubiquitinated.
  • 35. Activation of ubiquitin • Activated by ubiquitin E-1 (ubiquitin activating enzyme), in energy dependent manner E-1 attach to ubiquitin at C- terminal. • Then, E-1 transfer to a ‘cysteine residue’ present on an E-2 (ubiquitin conjugating enzyme). • Finally E-3 (ubiquitin ligase)transferred the activated ubiquitin from E-2 to a lysine amino acid residue of its target protein, forming an isopeptide bond.
  • 36.
  • 37. Attractions: • Cell cycle • Checkpoints • Activation/inactivation of cyclin-cdks complex • Rb protein • P53 protein • Ubiquitin mediated proteasomal degradation